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Eclinicalmedicine: Contents Lists Available at
Eclinicalmedicine: Contents Lists Available at
EClinicalMedicine
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Targeting the HIV Epidemic in South Africa: The Need for Testing and
Linkage to Care in Emergency Departments
Bhakti Hansotia,∗, George Mwinnyaaa,b,1, Elizabeth Hahna,1, Aditi Raoa,1, John Blackc,d,
Victoria Chena, Kathryn Clarka, William Clarkea, Anna L. Eisenbergb, Reinaldo Fernandeza,
Joshua Iruedoc, Oliver Laeyendeckera,b, Roshen Maharajc,e, Pamela Mdaf, Jernelle Millera,
Nomzamo Mvandabac, Yandisa Nyanisac, Steven J. Reynoldsa,b, Andrew D. Redda,b,
Sofia Ryana, David F. Steadc,g, Lee A. Wallish, Thomas C. Quinna,b
a
The Johns Hopkins University, 1800 Orleans St, Baltimore, MD 21287, USA
b
Division of Intramural Research, National Institute of Allergy and Infectious Diseases, 31 Center Dr # 7A03, Bethesda, MD 20892, USA
c
Faculty of Health Sciences, Walter Sisulu University, Umtata Part 1, Mthatha, South Africa
d
Department of Medicine, Livingstone Hospital, Stanford Road, Korsten, Port Elizabeth 6020, South Africa
e
Department of Emergency Medicine, Livingstone Hospital, Stanford Road, Korsten, Port Elizabeth 6020, South Africa
f
Nelson Mandela Hospital Clinical Research Unit, Sisson St, Fort Gale, Mthatha 5100, South Africa
g
Department of Medicine, Frere Hospital, Amalinda Main Rd, Braelyn, East London 5201, South Africa
h
Division of Emergency Medicine, University of Cape Town, Main Rd, Observatory, Cape Town 7925, South Africa
a r t i c l e i n f o a b s t r a c t
Article history: Background: The Eastern Cape province of South Africa has one of the highest burdens of HIV in the
Received 13 May 2019 world. Emergency Departments (EDs) can serve as optimal clinical sites for the identification of new HIV
Revised 12 August 2019
infections and entry into care. We sought to determine the current burden of HIV disease among ED
Accepted 12 August 2019
patients in the Eastern Cape.
Available online 19 August 2019
Methods: We conducted a prospective cross-sectional observational study in the EDs of three Hospitals
Keywords: in the Eastern Cape province of South Africa from June 2017 to July 2018. All adult, non-critical patients
HIV testing presenting to the ED were systematically approached and offered a Point-Of-Care (POC) HIV test in accor-
HIV in men dance with South African guidelines. All HIV-positive individuals had their blood tested for the presence
South Africa of antiretroviral therapy (ART) and the presence of viral suppression (≤ 1000 copies/ml). HIV incidence
Emergency medicine was estimated using a multi-assay algorithm, validated for a subtype C epidemic.
HIV and trauma
Findings: Of the 2901 patients for whom HIV status was determined (either known HIV-positive or un-
derwent POC HIV testing), 811 (28.0%) were HIV positive, of which 234 (28.9%) were newly diagnosed.
HIV prevalence was higher in Mthatha [34% (388/1134) at Mthatha Regional Hospital and 28% (142/512)
at Nelson Mandela Academic Hospital], compared to Port Elizabeth [22% (281/1255) at Livingstone Hos-
pital]. HIV incidence was estimated at 4.5/100 person-years (95% CI: 2.4, 6.50) for women and 1.5 (CI
0.5, 2.5) for men. Of all HIV positive individuals tested for ART (585), 54% (316/585) tested positive for
the presence of ARTs, and for all HIV positive participants with viral load data (609), 49% (299/609) were
found to be virally suppressed.
Interpretation: Our study not only observed a high prevalence and incidence of HIV among ED patients
but also highlights significant attrition along the HIV care cascade for HIV positive individuals. Further-
more, despite developing an optimal testing environment, we were only able to enrol a small sub-set of
the ED population. Given the high HIV prevalence and high attrition in the ED population, HIV services
in the ED should also develop strategies that can accommodate large testing volumes and ART initiation.
© 2019 Published by Elsevier Ltd. This is an open access article under the CC BY-NC-ND license.
(http://creativecommons.org/licenses/by-nc-nd/4.0/)
∗
Corresponding author.
E-mail addresses: [email protected] (B. Hansoti), [email protected] Laeyendecker), [email protected] (J. Miller), [email protected] (S.J. Reynolds),
(G. Mwinnyaa), [email protected] (E. Hahn), [email protected] (A. Rao), [email protected] (A.D. Redd), [email protected] (S. Ryan), [email protected]
[email protected] (K. Clark), [email protected] (W. Clarke), [email protected] (L.A. Wallis), [email protected] (T.C. Quinn).
1
(A.L. Eisenberg), [email protected] (R. Fernandez), [email protected] (O. Indicates joint second author and equal contribution.
https://doi.org/10.1016/j.eclinm.2019.08.007
2589-5370/© 2019 Published by Elsevier Ltd. This is an open access article under the CC BY-NC-ND license. (http://creativecommons.org/licenses/by-nc-nd/4.0/)
B. Hansoti, G. Mwinnyaa and E. Hahn et al. / EClinicalMedicine 15 (2019) 14–22 15
Implications of all the available evidence This prospective cross-sectional observational study was con-
ducted in the ED in three hospitals in the Eastern Cape province
Policymakers both in South Africa and beyond should crit- between June 2017 and July 2018. Each hospital was sampled for
ically evaluate the need to implement and support ED-based a period of six weeks, during which all eligible patients, were ap-
HIV care if we are to meet the UNAIDS 90-90-90 targets. proached study staff and offered point-of-care (POC) HIV testing. In
However, ED-based HIV testing must be coupled with ART
addition, all previously known, and newly diagnosed HIV positive
initiation and linkage to care strategies, which will require
patients were requested to provide an additional blood sample for
innovative solutions for long term-sustainability and imple-
mentation. further laboratory testing.
Fig. 1. Overview of study population and enrollment in point-of-care testing and further laboratory analysis for HIV positive individuals across sites.
2.4. HIV Testing Intervention This testing algorithm has a window period of 248 days and has
been objectively compared to provide near-identical incidence es-
During the study period, HIV testing was implemented and con- timates observed in a longitudinal cohort [15].
ducted in accordance with the 2015 National HCT Guidelines. The
core recommendations of the national guidelines mandate an opt- 2.6. Demographic Data Collection
in testing approach requiring informed consent with extensive pre-
and post-test counselling in a confidential private setting. All study We collected additional patient-level information such as age,
staff were trained in rapid POC HIV testing and counselling, were sex, presenting complaint, the severity of illness, disposition, and
required to be fluent in English, Xhosa and/or Afrikaans and, com- previous diagnosis of HIV infection. The severity of illness was
pleted Good Clinical Practice (GCP) and data collection training. All quantified using the South African Triage Scale (SATS) [16]. Data
patients were first tested with the Advanced QualityTM Rapid Anti- were prospectively collected on case report forms that were
HIV 1 & 2 test (InTec Products, Inc, Xiamen, China). Non-reactive scanned and entered using intelligent character recognition (ICR)
specimens were considered HIV-negative. All reactive specimens DataFax© software (DataFax, Clinical DataFax Systems Inc., Hamil-
were confirmed using an ABONTM HIV 1/2/O Tri-line HIV Rapid ton, Ontario, Canada) and centrally double-verified by independent
Test (ABON Biopharm, Hangzhou, China). As per the 2015 HCT data technicians.
Guidelines [13], patients with two reactive rapid tests were con-
sidered to be HIV positive, and no further confirmatory testing was
2.7. Sample Size, Outcome Measures and Data Analysis
done. Patients with discordant results were referred for re-testing
using an ELISA at the local ARV clinic, but for the purpose of analy-
The 2012 South African National HIV prevalence study esti-
sis, they were classified as HIV negative. Patients were informed of
mated the HIV prevalence in the Eastern Cape to be 19.9% [6,9]. To
their HIV results immediately after testing completion. HIV nega-
detect a difference of greater than 5% from the baseline estimate of
tive patients were provided with standard post-test counselling on
19.9%, with a 95% confidence interval and power of 0.8, our study
the HIV prevention strategies, the window period and importance
needed to recruit at least 534 patients per study site. Based on the
of re-testing. HIV positive were provided with post-test counselling
ED volumes (approximately 100–150/day), we conservatively esti-
on linkage to care and a letter stating their results with directions
mated the ability to enrol between 15 and 20 patients per day and
to a local HIV clinic.
thus planned to recruit patients for a six-week duration per study
site.
2.5. Further Laboratory Testing Patients were defined as “HIV positive” if they self-reported
a previous diagnosis of HIV infection (i.e., “Known HV”) or were
All patients who self-reported as being HIV positive, or those “Newly Diagnosed with HIV” if they did not know their HIV sta-
who underwent POC testing and were identified as HIV positive, tus and then had two positive POC rapid HIV tests. Patients were
were further consented to provide a blood sample for labora- defined as “HIV negative” if they had a single negative POC rapid
tory testing. All tests were conducted based on sample availabil- HIV test. Patients were defined as “Unknown Status” if they were
ity. Serum was isolated and stored at −80 °C. Presence of any ART unaware of their status and refused a POC rapid HIV test.
drugs within serum samples was assessed using HPLC-High Res- The descriptive analysis explored the overall HIV prevalence,
olution Accurate Mass (HRAM) spectrometry [13]. Samples with the proportion of newly diagnosed patients, and the proportion of
sufficient volume were tested for HIV viral load using the Abbott patients on any ARTs and virally suppressed (VL < 1000 copies/ml).
m2000 RealTime System with a detection limit of 320 copies/mL. Comparisons of patient characteristics by HIV status were con-
(Abbott Park, IL), due to low volume testing algorithm, viral loads ducted using chi-squared tests. Log-binomial models were used to
(VL) < 1000 copies/ml were considered virally suppressed. Sam- estimate to estimate crude (unadjPR) and adjusted (adjPR) preva-
ples were also tested with a limiting-antigen avidity enzyme im- lence ratios. In situations where the log-binomial model failed to
munoassay (LAg-Avidity). Using a multi-assay algorithm, which has converge, modified Poisson regression with robust variance were
been validated for a subtype C epidemic [14]. Subjects with a VL used. The following independent variables, age group, sex, present-
> 1000 copies/ml, a Limiting Antigen avidity assay normalised op- ing complaint, time of testing, symptomology, and severity of sick-
tical density of < 2.8 and a Johns Hopkins modified BioRad Avidity ness were included in the multivariate model to examine the asso-
assay index result below 95% were considered recently infected. ciation between patient characteristics and attrition along the care
B. Hansoti, G. Mwinnyaa and E. Hahn et al. / EClinicalMedicine 15 (2019) 14–22 17
Table 1
Characteristics of All Participants by Testing Site.
Age
< 20 36 (5.79%) 62 (4.93%) 61 (3.68%) 159 (4.50%)
20–25 141 (22.67%) 252 (20.03%) 259 (15.63%) 652 (18.43%)
26–35 174 (27.97%) 335 (26.63%) 491 (29.63%) 1000 (28.27%)
36–45 79 (12.70%) 192 (15.26%) 337 (20.34%) 608 (17.19%)
46–55 55 (8.84%) 116 (9.22%) 260 (15.69%) 431 (12.19%)
56 + 137 (22.03%) 301 (23.93%) 249 (15.03%) 687 (19.42%)
Sex
Female 247 (39.71%) 719 (57.15%) 793 (47.86%) 1759 (49.73%)
Male 375 (60.29%) 539 (42.85%) 864 (52.14%) 1778 (50.27%)
Presenting compliant
Medical 360 (57.88%) 912 (72.50%) 755 (45.56%) 2027 (57.31%)
Trauma 262 (42.12%) 346 (27.50%) 902 (54.44%) 1510 (42.69%)
Time of presentation
Routine hours 249 (40.03%) 540 (42.93%) 625 (37.72%) 1414 (39.98%)
Out of hours 373 (59.97%) 718 (57.07%) 1032 (62.28%) 2123 (60.02%)
SATSa
Emergency 0 (0.0%) 0 (0.0%) 31 (1.87%) 31 (0.88%)
Very urgent 186 (29.9%) 358 (28.46%) 114 (6.88%) 658 (18.60%)
Urgent 401 (64.47%) 868 (69.0%) 839 (50.63%) 2108 (59.60%)
Routine 35 (5.63%) 32 (2.54%) 673 (40.62%) 740 (20.92%)
Deceased 0 (0.0%) 0 (0.0%) 0 (0.0%) 0 (0.0%)
Disposition
Death 0 (0.0%) 8 (0.64%) 1 (0.06%) 9 (0.25%)
Admission 305 (49.04%) 305 (24.24%) 142 (8.57%) 752 (21.26%)
Emergent surgery 101 (16.24%) 3 (0.24%) 1 (0.06%) 105 (2.97%)
ICU admission 1 (0.16%) 1 (0.08%) 1 (0.06%) 3 (0.08%)
Transfer 54 (8.68%) 58 (4.61%) 278 (16.78%) 390 (11.03%)
Discharge 141 (22.67%) 769 (61.13%) 1120 (67.59%) 2030 (57.39%)
Absconded 3 (0.48%) 1 (0.08%) 103 (6.22%) 107 (3.03%)
Unassigned 17 (2.73%) 113 (8.98%) 11 (0.66%) 141 (3.99%)
Consent to POC testing
Declined (known positive)d 98 (15.59%) 253 (20.03%) 197 (11.95%) 548 (15.47%)
Declined (unknown status)e 110 (17.86%) 124 (9.86%) 402 (24.20%) 636 (17.95%)
Accepted test 414 (66.72%) 881 (70.11%) 1058 (63.85%) 2353 (66.58%)
HIV statusc
Known HIV 109 (17.52%) 262 (20.83%) 206 (12.43%) 577 (16.31%)
HIV negative 370 (59.49%) 746 (59.30%) 974 (58.78%) 2090 (59.09%)
Newly diagnosed HIV 33 (5.31%) 126 (10.02%) 75 (4.53%) 234 (6.62%)
Unknownb 110 (17.68%) 124 (9.86%) 402 (24.26%) 636 (17.98%)
a
South African Triage Score (SATS).
b
Unknown status is defined as those who were not known to be HIV positive, and refused to enrol in the study and undergo POC testing.
c
The number of patients with a documented test (N) was used as the denominator when calculating the proportion with a positive or negative result (n).
d
Declined - known positive defined as marking known positive but not consenting to test.
e
Declined – unknown defined as no known HIV diagnosis and did not consent to test.
cascade for those that are HIV positive. HIV incidence and 95% CI at approximately 66.5% (range: 63.9%–70.0%) (Table 1). The age dis-
estimates were calculated using methods previously described us- tribution remained consistent across all sites, and most ED patients
ing a window period of 248 days and a false recent ratio of 0% [14]. were under the age of 35 [51.2% (1811/3537)] (Table 1). The two
tertiary care facilities (NMAH and LH) provided care to a higher
2.8. Ethical Considerations proportion of male patients (60.3% and 52.1% respectively) and to
a higher proportion of trauma patients (42.1% and 54.4% respec-
The study was approved by the Johns Hopkins University School tively).
of Medicine Institutional Review Board, the University of Cape
Town Human Research Ethics Committee (HREC), and the Walter 3.2. HIV Prevalence
Sisulu University HREC. Written consent was obtained from all par-
ticipants for the collection of demographic data, POC HIV testing, Of the 2901 patients for whom HIV status was determined
and sample collection if HIV positive. (either known HIV-positive or underwent POC HIV testing), 811
(28.0%) were HIV positive, of which 234 (28.9%) had a new diag-
3. Results nosis. HIV prevalence was higher in Mthatha (34% [388/1134] at
MRH, and 28% [142/512] at NMAH), compared to Port Elizabeth
3.1. Overall Study Characteristics (22% [281/1255]) (Table 1). The prevalence of HIV was significantly
higher in females (n = 509, 35.3%) compared to males (n = 302,
Over the study period, a total of 3537 patients were approached 20.7%) (χ 2 (df 1, N = 2901), p < 0.001). HIV prevalence was highest
across all sites, of which 2901 enrolled and had their HIV status in females aged 36–45 years (55.4%; 95% CI: 49.0–61.5), and sec-
determined (Fig. 1). The number of patients approached varied by ond highest in females aged 26–35 years (49.6%; 95% CI: 44.5–54.7)
site: LH (n = 1657); MRH (n = 1258); and NMAH (n = 622), however (Fig. 2a). The peak prevalence in males was highest at 34.8% (95%
acceptance of HIV testing remained fairly even across all three sites CI: 29.3, 40.9) also in the 36–45 years age category. Medical pa-
18 B. Hansoti, G. Mwinnyaa and E. Hahn et al. / EClinicalMedicine 15 (2019) 14–22
Fig. 2. HIV prevalence, newly diagnosed, ARV presence and viral suppression by age and gender.
tients had a higher prevalence of HIV infection (34% [586/1723]) an independent risk factor for not being virally suppressed (adj.PR
as did patients who were sicker (defined as SATS ‘emergency’/‘very 1.22; 95% CI: 1.04, 1.42) (Table 3).
urgent’) (27% [619/2314]), and those that were subsequently admit-
ted (32% [332/1026]) (Table 2). 3.5. Care Continuum
Table 2
Characteristics of participants with a determined HIV status across all sites.
Age
< 20 132 121 (5.79%) 4 (0.69%) 7 (2.99%) < 0.001
20–25 542 431 (20.62%) 65 (11.27%) 46 (19.66%)
26–35 816 526 (25.17%) 192 (33.28%) 98 (41.88%)
36–45 500 276 (13.21%) 175 (30.33%) 49 (20.94%)
46–55 358 253 (12.10%) 91 (15.77%) 14 (5.98%)
56 + 553 483 (23.11%) 50 (8.66%) 20 (8.55%)
Sex
Female 1443 934 (44.69%) 399 (69.15%) 110 (47.01%) < 0.001
Male 1458 1156 (55.31%) 178 (30.85%) 124 (52.99%)
Presenting compliant
Medical 1723 1137 (54.40%) 430 (74.52%) 156 (66.67%) < 0.001
Trauma 1178 953 (45.60%) 147 (25.48%) 78 (33.33%)
Time of presentation
Routine hours 1157 812 (38.85%) 252 (43.67%) 93 (39.74%) 0.111
Out of hours 1744 1278 (61.15%) 325 (56.33%) 141 (60.26%)
SATSa
Emergency 23 17 (0.81%) 5 (0.87%) 1 (0.43%) < 0.001
Very urgent 564 378 (18.09%) 130 (22.53%) 56 (23.93%)
Urgent 1745 1235 (59.09%) 363 (62.91%) 147 (62.82%)
Routine 569 460 (22.01%) 79 (13.69%) 30 (12.82%)
Disposition
Death 7 4 (0.19%) 3 (0.52%) 0 (0.0%)
Admission 639 419 (20.05%) 165 (28.60%) 55 (23.50%)
Emergent surgery 87 65 (3.11%) 16 (2.77%) 6 (2.56%) < 0.001
ICU admission 3 2 (0.09%) 0 (0.0%) 1 (0.43%)
Transfer 297 208 (9.95%) 68 (11.79%) 21 (8.97%)
Discharge 1659 1259 (60.24%) 272 (47.14%) 128 (54.70%)
Absconded 80 66 (3.16%) 9 (1.56%) 5 (2.14%)
Unassigned 129 67 (3.21%) 44 (7.62%) 18 (7.69%)
a
The number of patients with a documented test (N) was used as the denominator when calculating the proportion with a positive or negative result (n).
achievement of the 90–90-90 targets and incidence estimates [17]. are significantly under-represented in HIV testing and treatment
Per the HSRC estimates, 85% of people aged 15–64 years in South services–both in sub-Saharan Africa and globally [21]. Targeting
Africa who are living with HIV know their HIV status, 71% are men has the potential to significantly impact HIV-related mortal-
receiving ART, and 62.3% are virally suppressed [17]. In contrast, ity, incidence, and economic costs [22]. Due to men’s vastly dif-
our study data revealed that 71.1% of ED patients were aware of ferent health-seeking behaviours (women are more likely to seek
their status, 54% were positive for ARTs, and 49% were virally sup- healthcare), most facility-based programs will miss males [21]. Fur-
pressed. Given the attrition along the care cascade and the high thermore, most community-based interventions (such as commu-
number of young patients with undiagnosed infection, it is not nity HIV-care providers), fail to capture young men, as evidenced
surprising that the cross-sectional incidence estimate in our pop- by the poor recruitment of males in the HVTN071 (PopART) studies
ulation was higher than the incidence nationally reported by the in South Africa and Zambia [23]. The ED provides a clinical venue
HSRC [17]. The estimated incidence yielded by our ED-based study where men, who would otherwise be missed, can be engaged for
was 2.8 per 100 person-years (4.5 among females and 1.5 among counselling, testing, and linkage to care.
males) compared to the HSRC reported incidence of 0.79 per 100 Lastly, this study also exemplifies the well-known reality that
person-years (0.93 among females and 0.69 among males) [17]. high incidence and attrition along the care cascade go hand in
Numerous studies describe the need to target resources to ar- hand. The ANRS 12249 TasP trial in South Africa evaluated the im-
eas of high HIV burden and transmission, referred to as “hotspots” pact of Universal test and treat (UTT) on the HIV epidemic and
[18,19]. The ED has been identified in this study as an additional identified an absence of a lowering of HIV incidence in UTT clus-
hotspot that is often missed during the implementation of univer- ters [24]. They hypothesise that a lack of incidence reduction most
sal test and treat policies where the implementation of targeted likely resulted from poor linkage to care in the study population
HIV care strategies could have a substantial impact on HIV trans- [24]. While the ED is a strategic venue in which to target HIV test-
mission in areas of high HIV prevalence. Studies outside of South ing, it also is a complex clinical environment that provides care to
Africa have called for the implementation of routine testing and vulnerable patients, most of whom do not routinely access health-
counselling in the ED after finding high rates of testing acceptance care services. Innovative solutions must be sought, not only pro-
among ED patients, thereby catching significant numbers of undi- vide HIV services, but also ART initiation and linkage to care. Un-
agnosed HIV infections. A study in Uganda demonstrated that 76% derstanding the clinical setting and the care cascade will help in-
of HIV-positive individuals had not received HIV/AIDS care (defined form the design of tailored HIV services for ED patients.
as prevention and testing messages, HAART, or co-trimoxazole pro- The first challenge to implementing services in the ED is the
phylaxis) prior to enrolment in the ED-based HIV testing study high volume of patients and operational hours of the ED. Patients
[20]. For this reason, the ED is a prime location to identify un- seeking care are generally in favour of making HIV testing a routine
diagnosed HIV-positive patients and out-of-care HIV individuals to part of medical care [25]. Furthermore, by routinely offering HIV
improve capture toward the 90-90-90 targets. testing, the test will become normalised, decreasing stigma and
In addition to being hotspots, EDs capture the key and of- removing highly personal prerequisite discussions about the risk
ten missed demographic of young men. Evidence shows that men of HIV infection. The challenge remains how best to implement
20 B. Hansoti, G. Mwinnyaa and E. Hahn et al. / EClinicalMedicine 15 (2019) 14–22
routine testing in a complex clinical care environment, including patterns, same-day initiation, and point-of-care, CD4 and viral load
ensuring confidentiality, dignity, and availability of care and treat- testing should be explored in the ED [32]. Lastly, our study does
ment services after a new HIV diagnosis. Several studies have dis- not directly address retention in care. We did find, however, that
cussed opt-in versus opt-out testing approaches [26]. Another ap- known HIV positive male patients in the ED were significantly less
proach is to evaluate the utility of HIV self-testing and testing likely to be on ARTs and/or virally suppressed. One of the main
kiosks in the ED, which may combat the challenges around vol- weaknesses of this approach is getting HIV positive patients to link
umes and lack of HIV counsellors [27]. However, these approaches to care. Several studies in high resource settings have successful in-
only decrease the burden of the initial time for consent; the time tegrated mental health screening, violence screening and substance
for completing the test, interpreting results and providing referral abuse screening, with promising linkage to care outcomes [33,34].
services still remains. Additionally, a study from the United States There are a limited number of such studies in South Africa; how-
examined the effect of mandatory HIV screening in ED patients ever, there have been promising reports for pioneering screening
and found an increase in patient wait times, with the potential and brief interventions for substance use in South African emer-
for an increase in patients absconding [28]. It is likely that hybrid gency care settings [35–37]. ED-based HIV care would need to ad-
models will need to be developed that combine both self-testing dress the known challenges of linkage and retention, such a loca-
and provider-initiated testing approaches, with 24-hour access to tion and access to care, in order to maximise impact. Innovative
counsellors and ART initiation teams. solutions targeted to male patients, such as video-based program-
ART initiation and linkage to care is a second challenge. A re- ming, linkages to social networks and community-based support
cent modelling study, in South Africa, demonstrated that it takes programs should be explored [22].
on average 4.9 years for 50% of HIV seroconverters to be linked to
care (95% CI 4.2–5.7) [29]. Furthermore, they identified that men 5. Conclusion
and participants aged less than 30 years were found to have the
lowest rates of linkage-to-care [29]. Similarly, our study identified Emergency Departments provide care to large volumes of HIV
that young male patients were independently at higher risk of not positive individuals who are at high risk of attrition along the care
being on ARTs and not being virally suppressed. A potential solu- cascade. Furthermore, they are a venue to capture young men,
tion to this, within a healthcare context, is same-day ART initia- often missed by current avenues of HIV service delivery. Beyond
tion. The CASCADE study in South Africa found that offering same- their role in surveillance of the HIV epidemic, emergency depart-
day home-based ART initiation to individuals who tested positive ments should develop innovative HIV testing and linkage to care
during home-based HIV testing, compared with usual care and strategies that in particular meet the needs of young men who do
standard clinic referral, significantly increased linkage to care at not routinely access clinic-based health services.
3 months and HIV viral suppression at 12 months [30]. Same-day
ART initiation would need to be supported by clinical algorithms 5.1. Limitations
such as the Simplified Algorithm for Treatment Eligibility (“SLATE”)
and will require training and implementation support [31]. Given This was a cross-sectional study, and thus, there are a num-
the ED population of young males and the challenges of referral ber of limitations that need to be addressed. The lack of elec-
Table 4
Characteristics of participants by time of infection as determined by MAA test.
Newly diagnosed, not a recent infection(n = 186) (%) Newly diagnosed, recent HIV infection(n = 21) (%)a p-Value
Age
< 20 4 (66.67%) 2 (33.33%) 0.332
20–25 38 (92.68%) 3 (7.32%)
26–35 81 (92.05%) 7 (7.95%)
36–45 36 (87.80%) 5 (12.20%)
46–55 13 (92.86%) 1 (7.14%)
56 + 14 (82.35%) 3 (17.65%)
Sex
Female 86 (85.15%) 15 (14.85%) 0.029
Male 100 (94.34%) 6 (5.66%)
Presenting compliant
Medical 126 (89.36%) 15 (10.64%) 0.731
Trauma 60 (90.91%) 6 (9.09%)
Time of presentation
Routine hours 77 (90.59%) 8 (9.41%) 0.771
Out of hours 109 (89.34%) 13 (10.66%)
SATSa
Emergency 1 (100%) 0 (0.00%) 0.452
Very urgent 43 (89.58%) 5 (10.42%)
Urgent 120 (91.60%) 11 (8.40%)
Routine 22 (81.48%) 5 (18.52%)
Disposition
Death 0 (0.00%) 0 (0.00%) 0.164
Admission 47 (92.16%) 4 (7.84%)
Emergent surgery 6 (100%) 0 (0.00%)
ICU admission 0 (0.00%) 1(100%)
Transfer 16 (84.21%) 3 (15.79%)
Discharge 102 (91.07%) 10 (8.93%)
Absconded 2 (50.00%) 2 (50.00%)
Unassigned 12 (85.71%) 2 (14.29%)
a
Note that 29 patients tested as recent using the MAA assay, however 8 of these patients also tested positive for ARVs and thus they have been excluded
from the analysis above.
B. Hansoti, G. Mwinnyaa and E. Hahn et al. / EClinicalMedicine 15 (2019) 14–22 21
1.22(1.04,1.42) 1.33(1.05,1.67)
1.07(0.91,1.27) 0.99(0.77,1.28)
0.98(0.84,1.15) 0.93(0.74,1.17)
1.06(0.89,1.27) 1.10(0.84,1.44)
0.61(0.29,1.31)
0.67(0.33,1.37)
0.32(0.14,0.76)
0.96(0.82,1.13) 0.90(0.70,1.16)
0.70(0.53,0.92) 0.63(0.44,0.91)
0.49(0.24,1.03)
0.24(0.11,0.54)
enter the ED made it difficult to capture all patients that presented
N = 609 (100%) Not virally suppressed UnadPR(95% CI) adjPR(95% CI) for care. Only patients that were approached by HIV counsellors
1.00
1.00
1.00
1.00
1.00
1.00
were included in the analysis, thus a significant proportion of pa-
tients were not captured i.e., those that were too sick for HIV test-
ing (i.e., SATS category ‘emergency’ or being resuscitated), unable
0.37(0.16,0.85)
0.64(0.30,1.34)
0.72(0.35,1.47)
0.55(0.26,1.14)
0.28(0.12,0.62)
to consent for HIV testing (i.e., under the age of 18 or present-
ing with altered mental status), or were not approached by HIV
1.00
1.00
1.00
1.00
1.00
1.00
counsellors (i.e., unable to be enrolled due to limitations in staffing
Prevalence of not being virally suppressed
53%(152/289)
51%(138/268)
50%(219/439)
50%(172/341)
50%(237/472)
55%(120/220)
64%(139/217)
54%(91/170)
53%(73/137)
38%(38/100)
49%(76/156)
33%(17/52)
56%(48/85)
24%(22/90)
sample.
Funding
289(47)
170(28)
268(44)
137(23)
472(78)
373(61)
439(72)
341(56)
100(16)
220(36)
217(36)
156(26)
9(1.48)
85(14)
90(15)
port.
1.00
1.00
1.00
1.00
1.00
1.00
Acknowledgments
0.44(0.26,0.74)
0.78(0.53,1.15)
0.71(0.49,1.03)
0.54(0.36,0.80)
0.23(0.15,0.45)
1.00
1.00
1.00
1.00
their dedication and hard work during the study; the research and
42% (151/363)
46%(119/256)
44%(187/423)
46%(206/446)
50%(109/220)
55%(113/205)
42%(64/152)
34%(17/50)
61%(51/84)
20%(17/85)
162(28)
256(44)
268(46)
329(56)
449(77)
136(23)
363(62)
423(72)
152(26)
220(38)
205(35)
9(1.54)
85(15)
50(9)
1.30(1.04,1.63) 1.22(0.91,1.64)
1.22(0.96,1.55) 1.26(0.94,1.71)
0.39(0.17,0.94)
1.12(0.90,1.40) 1.07(0.82,1.39)
1.04(0.81,1.33) 1.07(0.78,1.45)
0.87(0.61,1.24) 0.84(0.56,1.27)
0.66(0.30,1.48)
0.48(0.22,1.05)
0.32(0.14,0.71)
0.18(0.07,0.45)
N = 811 (100%) Newly diagnosed UnadPR(95% CI) adjPR(95% CI)
Author Contributions
1.00
1.00
1.00
1.00
1.00
1.00
S Ryan, A Rao, VC, JI, PM, JB, RM, NM, YN, AE, JM, RF, WC made
substantial contributions to the acquisition of Data; BH, GM, EH,
Prevalence of being unaware of HIV infection
1.00
1.00
1.00
1.00
1.00
1.00
29%(177/619)
32%(126/388)
30%(141/466)
41% (46/111)
35%(78/225)
27%(93/345)
34%(98/290)
22%(49/224)
30%(57/192)
23%(33/142)
13%(14/105)
27%(75/281)
29%(20/70)
66% (7/11)
225(28)
345(43)
586(72)
466(57)
619(76)
192(24)
281(35)
388(48)
142(18)
70(9)
Time of presentation
//doi.org/10.1016/j.eclinm.2019.08.007.
Out of hours
Livingstone
References
Very sick
9-5/M-F
Medical
Trauma
Female
NMAH
25–35
35–45
45–55
20–25
MRH
Male
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